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首页> 外文期刊>Clinical and applied thrombosis/hemostasis : >Tissue Factor-Mediated Activation of the Prothrombin Complex Concentrate (PCC) is Differently Inhibited by Dabigatran, Rivaroxaban, and Apixaban: Potential Clinical Implication
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Tissue Factor-Mediated Activation of the Prothrombin Complex Concentrate (PCC) is Differently Inhibited by Dabigatran, Rivaroxaban, and Apixaban: Potential Clinical Implication

机译:组织因子介导的凝血酶原复合物浓缩物(PCC)的激活受达比加群,利伐沙班和阿哌沙班的抑制不同:潜在的临床意义

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摘要

Currently, several newer oral anticoagulants namely dabigatran (anti-IIa), rivaroxaban (anti-Xa), and apixaban are available for various clinical implications. Another oral anti-Xa edoxaban is under development. A parenteral anti-Xa drug namely otamixaban is also under development for cardiovascular interventions. Bleeding complications have been reported in the new oral anticoagulants and have been managed by conventional approaches with limited success. Prothrombin complex concentrates (PCCs) are reported to neutralize the anticoagulant activity of these agents. The PCCs are also able to generate endogenous factor Xa and IIa along with other proteases that are capable of neutralizing the circulating anti-Xa or anti-IIa activities of the newer anticoagulants. The generation of Xa and IIa is also dependent on the type of tissue factor available for their activation. These reported studies suggest that different tissue factors differentially activate a PCC namely Profilnine SD. Furthermore, dabigatran differs from rivaroxaban and other factor Xa inhibitors in its inhibitory profile.
机译:当前,几种较新的口服抗凝药,即达比加群(抗IIa),利伐沙班(抗Xa)和阿哌沙班可用于多种临床用途。另一种口服抗Xa edoxaban正在开发中。肠胃外抗Xa药物otamixaban也正在开发中,用于心血管干预。在新的口服抗凝剂中已经报道了出血并发症,并且已经通过常规方法进行了治疗,但效果有限。凝血酶原复合物浓缩物(PCCs)据报道可中和这些药物的抗凝活性。 PCC还能够产生内源性因子Xa和IIa以及能够中和新型抗凝剂循环中的抗Xa或抗IIa活性的其他蛋白酶。 Xa和IIa的产生还取决于可用于其活化的组织因子的类型。这些报道的研究表明,不同的组织因子差异地激活PCC,即Profilnine SD。此外,达比加群与利伐沙班和其他Xa因子抑制剂的抑制特性不同。

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